TY - JOUR
T1 - Modeling Borna Disease Virus in Vitro Spread Reveals the Mode of Antiviral Effect Conferred by an Endogenous Bornavirus-Like Element
AU - Kim, Kwang Su
AU - Yamamoto, Yusuke
AU - Nakaoka, Shinji
AU - Tomonaga, Keizo
AU - Iwami, Shingo
AU - Honda, Tomoyuki
N1 - Funding Information:
AMED CREST JP19gm1310002 (to S.I.), AMED J-PRIDE JP19fm0208006s0103 (to S.I.), JP19fm0208014h (to K.T. and S.I.), and JP19fm0208019h0103 (to S.I.), AMED Research Program on HIV/AIDS JP19fk0410023s0101 (to S.I.), Research Program on Emerging and Re-emerging Infectious Diseases JP19fk0108050h0003 (to S.I.), Program for Basic and Clinical Research on Hepatitis JP19fk0210036h0502 (to S.I.), Program on the Innovative Development and the Application of New Drugs for Hepatitis B JP19fk0310114h0103 (to S.I.), JSPS Core-to-Core Program, JST MIRAI (to S.I.), JST CREST (to S.I.), Mitsui Life Social Welfare Foundation (to S.I.), Shin-Nihon of Advanced Medical Research (to S.I.), Suzuken Memorial Foundation (to S.I.), Life Science Foundation of Japan (to S.I.), SECOM Science and Technology Foundation (to S.I.), The Japan Prize Foundation (to S.I.), Toyota Physical and Chemical Research Institute (to S.I.), the Basic Science Research Program through the National Research Foundation of Korea funded by Ministry of Education grant 2019R1A6A3A12031316 (to K.S.K.), the Shimizu Foundation for Immunology and Neuroscience Grant for 2015 (T.H.), and the Cooperative Research Program (Joint Usage/Research Center program) of the Institute for Frontier Life and Medical Sciences, Kyoto University (to T.H.).
Funding Information:
This study was supported in part by Grants-in-Aid for Scientific Research (KAKENHI) Scientific Research B JP18KT0018 (to S.I.), JP18H01139 (to S.I.), JP18H02664 (to T.H.), JP16H04845 (to S.I.), JP17H04083 (to K.T.), Challenging Research (Exploratory) JP18K19449 (to T.H.), JP19K22530 (to K.T.), Scientific Research on Innovative Areas JP19H04839 (to S.I.), JP18H05103 (to S.I.), JP16H06429 (to K.T.), JP16K21723 (to K.T.), and JP16H06430 (to K.T.),
Funding Information:
This study was supported in part by Grants-in-Aid for Scientific Research (KAKENHI) Scientific Research B JP18KT0018 (to S.I.), JP18H01139 (to S.I.), JP18H02664 (to T.H.), JP16H04845 (to S.I.), JP17H04083 (to K.T.), Challenging Research (Exploratory) JP18K19449 (to T.H.), JP19K22530 (to K.T.), Scientific Research on Innovative Areas JP19H04839 (to S.I.), JP18H05103 (to S.I.), JP16H06429 (to K.T.), JP16K21723 (to K.T.), and JP16H06430 (to K.T.), AMED CREST JP19gm1310002 (to S.I.), AMED J-PRIDE JP19fm0208006s0103 (to S.I.), JP19fm0208014h (to K.T. and S.I.), and JP19fm0208019h0103 (to S.I.), AMED Research Program on HIV/AIDS JP19fk0410023s0101 (to S.I.), Research Program on Emerging and Re-emerging Infectious Diseases JP19fk0108050h0003 (to S.I.), Program for Basic and Clinical Research on Hepatitis JP19fk0210036h0502 (to S.I.), Program on the Innovative Development and the Application of New Drugs for Hepatitis B JP19fk0310114h0103 (to S.I.), JSPS Core-to-Core Program, JST MIRAI (to S.I.), JST CREST (to S.I.), Mitsui Life Social Welfare Foundation (to S.I.), Shin-Nihon of Advanced Medical Research (to S.I.), Suzuken Memorial Foundation (to S.I.), Life Science Foundation of Japan (to S.I.), SECOM Science and Technology Foundation (to S.I.), The Japan Prize Foundation (to S.I.), Toyota Physical and Chemical Research Institute (to S.I.), the Basic Science Research Program through the National Research Foundation of Korea funded by Ministry of Education grant 2019R1A6A3A12031316 (to K.S.K.), the Shimizu Foundation for Immunology and Neuroscience Grant for 2015 (T.H.), and the Cooperative Research Program (Joint Usage/Research Center program) of the Institute for Frontier Life and Medical Sciences, Kyoto University (to T.H.).
Publisher Copyright:
Copyright © 2020 American Society for Microbiology. All Rights Reserved.
PY - 2020/10/14
Y1 - 2020/10/14
N2 - Endogenous retroviruses have demonstrated exaptation during long-term evolution with hosts, e.g., resulting in acquisition of antiviral effect on related extant viral infections. While empirical studies have found that an endogenous bornavirus-like element derived from viral nucleoprotein (itEBLN) in the ground squirrel genome shows antiviral effect on virus replication and de novo infection, the antiviral mechanism, dynamics, and quantitative effect of itEBLN remain unknown. In this study, we experimentally and theoretically investigated the dynamics of how an extant bornavirus, Borna disease virus 1 (BoDV-1), spreads and replicates in uninfected, BoDV-1-infected, and itEBLN-expressing cultured cells. Quantifying antiviral effect based on time course data sets, we found that the antiviral effects of itEBLN are estimated to be 75% and 34% on intercellular virus spread and intracellular virus replication, respectively. This discrepancy between intercellular virus spread and intracellular viral replication suggests that viral processes other than the replication of viral ribonucleoprotein complex (RNP) contributed to the suppression of virus spread in itEBLN-expressing cells. Because itEBLN binds to the BoDV-1 RNP, the suppression of viral RNP trafficking can be an attractive candidate explaining this discrepancy. IMPORTANCE Accumulating evidence suggests that some endogenous viral elements (EVEs), including endogenous retroviruses and endogenous nonretroviral virus elements, have acquired functions in the host as a result of long-term coevolution. Recently, an endogenous bornavirus-like element (itEBLN) found in the ground squirrel genome has been shown to have antiviral activity against exogenous bornavirus infection. In this study, we first quantified bornavirus spread in cultured cells and then calculated the antiviral activity of itEBLN on bornavirus infection. The calculated antiviral activity of itEBLN suggests its suppression of multiple processes in the viral life cycle. To our knowledge, this is the first study quantifying the antiviral activity of EVEs and speculating on a model of how some EVEs have acquired antiviral activity during host-virus arms races.
AB - Endogenous retroviruses have demonstrated exaptation during long-term evolution with hosts, e.g., resulting in acquisition of antiviral effect on related extant viral infections. While empirical studies have found that an endogenous bornavirus-like element derived from viral nucleoprotein (itEBLN) in the ground squirrel genome shows antiviral effect on virus replication and de novo infection, the antiviral mechanism, dynamics, and quantitative effect of itEBLN remain unknown. In this study, we experimentally and theoretically investigated the dynamics of how an extant bornavirus, Borna disease virus 1 (BoDV-1), spreads and replicates in uninfected, BoDV-1-infected, and itEBLN-expressing cultured cells. Quantifying antiviral effect based on time course data sets, we found that the antiviral effects of itEBLN are estimated to be 75% and 34% on intercellular virus spread and intracellular virus replication, respectively. This discrepancy between intercellular virus spread and intracellular viral replication suggests that viral processes other than the replication of viral ribonucleoprotein complex (RNP) contributed to the suppression of virus spread in itEBLN-expressing cells. Because itEBLN binds to the BoDV-1 RNP, the suppression of viral RNP trafficking can be an attractive candidate explaining this discrepancy. IMPORTANCE Accumulating evidence suggests that some endogenous viral elements (EVEs), including endogenous retroviruses and endogenous nonretroviral virus elements, have acquired functions in the host as a result of long-term coevolution. Recently, an endogenous bornavirus-like element (itEBLN) found in the ground squirrel genome has been shown to have antiviral activity against exogenous bornavirus infection. In this study, we first quantified bornavirus spread in cultured cells and then calculated the antiviral activity of itEBLN on bornavirus infection. The calculated antiviral activity of itEBLN suggests its suppression of multiple processes in the viral life cycle. To our knowledge, this is the first study quantifying the antiviral activity of EVEs and speculating on a model of how some EVEs have acquired antiviral activity during host-virus arms races.
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U2 - 10.1128/JVI.01204-20
DO - 10.1128/JVI.01204-20
M3 - Article
C2 - 32817215
AN - SCOPUS:85093538564
SN - 0022-538X
VL - 94
JO - Journal of Virology
JF - Journal of Virology
IS - 21
M1 - e01204-20
ER -